Carboplatin Explained

Verifiedfields:changed
Verifiedrevid:460018795
Tradename:Paraplatin, others
Routes Of Administration:Intravenous
Atc Prefix:L01
Atc Suffix:XA02
Legal Ca:Rx-only
Legal Ca Comment:[1]
Legal Status:Rx-only
Bioavailability:complete
Protein Bound:Very low
Elimination Half-Life:1.1-2 hours
Excretion:Kidney
Cas Number:41575-94-4
Pubchem:498142
Drugbank:DB00958
Chemspiderid:8514637
Unii:BG3F62OND5
Kegg:D01363
Chebi:31355
Chembl:288376
Iupac Name:cis-diammine(cyclobutane-1,1-dicarboxylate-O,O)platinum(II)
C:6
H:12
N:2
O:4
Pt:1
Smiles:C1CC2(C1)C(=O)O[Pt-2]([NH3+])([NH3+])OC2=O
Stdinchi:1S/C6H8O4.2H3N.Pt/c7-4(8)6(5(9)10)2-1-3-6;;;/h1-3H2,(H,7,8)(H,9,10);2*1H3;/q;;;+2/p-2
Stdinchikey:OLESAACUTLOWQZ-UHFFFAOYSA-L

Carboplatin, sold under the brand name Paraplatin among others, is a chemotherapy medication used to treat a number of forms of cancer. This includes ovarian cancer, lung cancer, head and neck cancer, brain cancer, and neuroblastoma. It is used by injection into a vein.[2]

Side effects generally occur.[2] Common side effects include low blood cell levels, nausea, and electrolyte problems.[3] [2] Other serious side effects include allergic reactions and mutagenesis. It may be carcinogenic, but further research is needed to confirm this. Use during pregnancy may result in harm to the baby. Carboplatin is in the platinum-based antineoplastic family of medications and works by interfering with duplication of DNA.[2] [4]

Carboplatin was developed as a less toxic analogue of cisplatin. It was patented in 1972 and approved for medical use in 1989.[5] It is on the 2023 World Health Organization's List of Essential Medicines.[6]

Medical uses

Carboplatin is used to treat a number of forms of cancer. This includes ovarian cancer, lung cancer, head and neck cancer, brain cancer, and neuroblastoma. It may be used for some types of testicular cancer but cisplatin is generally more effective.[2] It has also been used to treat triple-negative breast cancer.

Side effects

Relative to cisplatin, the greatest benefit of carboplatin is its reduced side effects, particularly the elimination of nephrotoxic effects. Nausea and vomiting are less severe and more easily controlled.[7]

The main drawback of carboplatin is its myelosuppressive effect. This causes the blood cell and platelet output of bone marrow in the body to decrease quite dramatically, sometimes as low as 10% of its usual production levels. The nadir of this myelosuppression usually occurs 21–28 days after the first treatment, after which the blood cell and platelet levels in the blood begin to stabilize, often coming close to its pre-carboplatin levels. This decrease in white blood cells (neutropenia) can cause complications, and is sometimes treated with drugs like filgrastim. The most notable complication of neutropenia is increased probability of infection by opportunistic organisms, which necessitates hospital readmission and treatment with antibiotics.

Mechanism of action

Carboplatin differs from cisplatin in that it has a bidentate dicarboxylate (the ligand is cyclobutane dicarboxylate, CBDCA) in place of the two chloride ligands. Both drugs are alkylating agents. CBDCA and chloride are the leaving groups in these respective drugs Carboplatin exhibits slower aquation (replacement of CBDCA by water) and thus slower DNA binding kinetics, although it forms the same reaction products in vitro at equivalent doses with cisplatin. Unlike cisplatin, carboplatin may be susceptible to alternative mechanisms. Some results show that cisplatin and carboplatin cause different morphological changes in MCF-7 cell lines while exerting their cytotoxic behaviour.[8] The diminished reactivity limits protein-carboplatin complexes, which are excreted. The lower excretion rate of carboplatin means that more is retained in the body, and hence its effects are longer lasting (a retention half-life of 30 hours for carboplatin, compared to 1.5-3.6 hours in the case of cisplatin).

Like cisplatin, carboplatin binds to and cross-links DNA, interfering with the replication and suppressing growth of the cancer cell.[9] [10]

Dose

Calvert's formula is used to calculate the dose of carboplatin. It considers the creatinine clearance and the desired area under curve.[11] After 24 hours, close to 70% of carboplatin is excreted in the urine unchanged. This means that the dose of carboplatin must be adjusted for any impairment in kidney function.[12]

Calvert formula:

Dose(mg)=AUC(GFR+25)

The typical area under the curve (AUC) for carboplatin ranges from 3-7 (mg/ml)*min.

Synthesis

Cisplatin reacts with silver nitrate and then cyclobutan-1,1-dicarboxylic acid to form carboplatin.[13]

History

Carboplatin, a cisplatin analogue, was developed by Bristol Myers Squibb and the Institute of Cancer Research in order to reduce the toxicity of cis platin.[14] [15] It gained U.S. Food and Drug Administration (FDA) approval for carboplatin, under the brand name Paraplatin, in March 1989. Starting in October 2004, generic versions of the drug became available.

Research

Carboplatin has also been used for adjuvant therapy of stage 1 seminomatous testicular cancer. Research has indicated that it is not less effective than adjuvant radiotherapy for this treatment, while having fewer side effects.[16] This has led to carboplatin based adjuvant therapy being generally preferred over adjuvant radiotherapy in clinical practice.[17]

Carboplatin combined with hexadecyl chain and polyethylene glycol appears to have increased liposolubility and PEGylation. This is useful in chemotherapy, specifically for non-small cell lung cancer.[18]

Further reading

Notes and References

  1. Web site: Product monograph brand safety updates . . 7 July 2016 . 3 April 2024.
  2. Web site: Carboplatin. The American Society of Health-System Pharmacists. 8 December 2016. live. https://web.archive.org/web/20161221012052/https://www.drugs.com/monograph/carboplatin.html. 21 December 2016.
  3. Oun R, Moussa YE, Wheate NJ . The side effects of platinum-based chemotherapy drugs: a review for chemists . Dalton Transactions . 47 . 19 . 6645–6653 . May 2018 . 29632935 . 10.1039/c8dt00838h .
  4. Apps MG, Choi EH, Wheate NJ . The state-of-play and future of platinum drugs . Endocrine-Related Cancer . 22 . 4 . R219–R233 . August 2015 . 26113607 . 10.1530/ERC-15-0237 . free . 2123/24426 . free .
  5. Book: Fischer J, Ganellin CR . Analogue-based Drug Discovery. 2006. John Wiley & Sons. 9783527607495. 513. en. live. https://web.archive.org/web/20161220163817/https://books.google.ca/books?id=FjKfqkaKkAAC&pg=PA513. 2016-12-20.
  6. Book: The selection and use of essential medicines 2023: web annex A: World Health Organization model list of essential medicines: 23rd list (2023) . ((World Health Organization)) . World Health Organization . 2023 . Geneva . 10665/371090 . WHO/MHP/HPS/EML/2023.02 . World Health Organization . free.
  7. Book: Manual of Hematopoietic Cell Transplantation and Cellular Therapies . Gulbis AM, Wallis WD . 2023 . 125–143 . 10 - Preparative Regimens Used in Hematopoietic Cell Transplantation and Chimeric Antigen Receptor T-Cell Therapies . Elsevier . 10.1016/B978-0-323-79833-4.00010-3. 9780323798334 .
  8. Natarajan G, Malathi R, Holler E . Increased DNA-binding activity of cis-1,1-cyclobutanedicarboxylatodiammineplatinum(II) (carboplatin) in the presence of nucleophiles and human breast cancer MCF-7 cell cytoplasmic extracts: activation theory revisited . Biochemical Pharmacology . 58 . 10 . 1625–1629 . November 1999 . 10535754 . 10.1016/S0006-2952(99)00250-6 .
  9. Noll DM, Mason TM, Miller PS . Formation and repair of interstrand cross-links in DNA . Chemical Reviews . 106 . 2 . 277–301 . February 2006 . 16464006 . 2505341 . 10.1021/cr040478b .
  10. Book: Encyclopedia of Respiratory Medicine . Edelman MJ, Rupard EJ . 2006 . 332–338 . TUMORS, MALIGNANT / Chemotherapeutic Agents . Academic Press . 10.1016/B0-12-370879-6/00409-9. 9780123708793 .
  11. Web site: New Guidelines for Carboplatin Dosing. O'Cearbhaill R, Sabbatini PS . September 1, 2012. Memorial Sloan Kettering Cancer Center. 2014-03-27 . live . https://web.archive.org/web/20141031014904/http://www.mskcc.org/cancer-care/clinical-update/new-guidelines-carboplatin-dosing . 2014-10-31 .
  12. Calvert AH, Newell DR, Gumbrell LA, O'Reilly S, Burnell M, Boxall FE, Siddik ZH, Judson IR, Gore ME, Wiltshaw E . 6 . Carboplatin dosage: prospective evaluation of a simple formula based on renal function . Journal of Clinical Oncology . 7 . 11 . 1748–1756 . November 1989 . 2681557 . 10.1200/JCO.1989.7.11.1748 .
  13. Book: Synthesis of Essential Drugs . Vardanyan RS, Hruby VJ . 2006 . 389–418 . 30 - Antineoplastics . Elsevier . 10.1016/B978-044452166-8/50030-3. 9780444521668 .
  14. Lebwohl D, Canetta R . 1998 . Clinical development of platinum complexes in cancer therapy: an historical perspective and an update . Eur J Cancer . 34 . 10 . 1522–34 . 10.1016/s0959-8049(98)00224-x . 9893623.
  15. Web site: Discovering early chemotherapy drugs . 2023-10-06 . Institute of Cancer Research.
  16. Oliver RT, Mason MD, Mead GM, von der Maase H, Rustin GJ, Joffe JK, de Wit R, Aass N, Graham JD, Coleman R, Kirk SJ, Stenning SP . 6 . Radiotherapy versus single-dose carboplatin in adjuvant treatment of stage I seminoma: a randomised trial . Lancet . 366 . 9482 . 293–300 . 2005 . 16039331 . 10.1016/S0140-6736(05)66984-X . 6001898 . free .
  17. Toner GC . Testicular cancer: Optimal management of stage I seminoma in 2015 . Nature Reviews. Urology . 12 . 5 . 249–251 . May 2015 . 25896179 . 10.1038/nrurol.2015.85 . 8072355 .
  18. Lang T, Li N, Zhang J, Li Y, Rong R, Fu Y . Prodrug-based nano-delivery strategy to improve the antitumor ability of carboplatin in vivo and in vitro . Drug Delivery . 28 . 1 . 1272–1280 . December 2021 . 34176381 . 8238065 . 10.1080/10717544.2021.1938754 .